Valdés Iris, Bernardo Lidice, Gil Lázaro, Pavón Alekis, Lazo Laura, López Carlos, Romero Yaremis, Menendez Ivón, Falcón Viviana, Betancourt Lázaro, Martín Jorge, Chinea Glay, Silva Ricardo, Guzmán María G, Guillén Gerardo, Hermida Lisset
Vaccine Division, Center for Genetic Engineering and Biotechnology (CIGB), Ave 31, P.O. Box 6162, Havana 6, 10 600, Cuba.
Virology. 2009 Nov 25;394(2):249-58. doi: 10.1016/j.virol.2009.08.029. Epub 2009 Sep 23.
Based on the immunogenicity of domain III from the Envelope protein of dengue virus as well as the proven protective capacity of the capsid antigen, we have designed a novel domain III-capsid chimeric protein with the goal of obtaining a molecule potentially able to induce both humoral and cell-mediated immunity (CMI). After expression of the recombinant gene in Escherichia coli, the domain III moiety retained its antigenicity as evaluated with anti-dengue sera. In order to explore alternatives for modulating the immunogenicity of the protein, it was mixed with oligodeoxynucleotides in order to obtain particulated aggregates and then immunologically evaluated in mice in comparison with non-aggregated controls. Although the humoral immune response induced by both forms of the protein was equivalent, the aggregated variant resulted in a much stronger CMI as measured by in vitro IFN-gamma secretion and protection experiments, mediated by CD4(+) and CD8(+) cells. The present work provides additional evidence in support for a crucial role of CMI in protection against dengue virus and describes a novel vaccine candidate against the disease based on a recombinant protein that can stimulate both arms of the acquired immune system.
基于登革病毒包膜蛋白结构域III的免疫原性以及衣壳抗原已证实的保护能力,我们设计了一种新型的结构域III - 衣壳嵌合蛋白,目的是获得一种可能能够诱导体液免疫和细胞介导免疫(CMI)的分子。在大肠杆菌中表达重组基因后,用抗登革热血清评估发现结构域III部分保留了其抗原性。为了探索调节该蛋白免疫原性的替代方法,将其与寡脱氧核苷酸混合以获得颗粒状聚集体,然后与未聚集的对照相比,在小鼠中进行免疫评估。尽管两种形式的蛋白诱导的体液免疫反应相当,但通过体外IFN - γ分泌和保护实验测量,聚集变体导致更强的CMI,由CD4(+)和CD8(+)细胞介导。本研究提供了额外的证据,支持CMI在预防登革病毒中的关键作用,并描述了一种基于重组蛋白的新型抗该疾病疫苗候选物,该重组蛋白可以刺激获得性免疫系统的两个分支。
